Trajectory of electrophilic attack on trisubstituted cyclopropanes - The

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J . Org. Chem. 1990,55, 4136-4144

Trajectory of Electrophilic Attack on Trisubstituted Cyclopropanes James M. Coxon,* Peter J. Steel,* and Barry I. Whittington Chemistry Department, University of Canterbury, Christchurch, New Zealand Received August 22, 1989

In the reactions of 2-exo-methyl-endo-tricyclo[3.2.1.0z~4]octane (1) and 2-ezo-methyl-endo-tricyclo[3.2.1.02-4]oct-6-ene(12) with both mercuric ion and proton, the electrophile attacks the cyclopropane moiety a t the corner with inversion. For the reactions with mercuric ion, the propensity toward inversion of Configuration a t the site of nucleophilic attack is accounted for in terms of the looseness of the transition state and the absence of substantial development of positive charge at the tertiary center. In contrast, the reactions with proton proceed with significant development of positive charge a t the tertiary center and occur with reduced regiospecificity and with attack of nucleophile being less stereospecific.

Introduction We have been interested for some time in the reaction of proton and mercuric ion with cyclopropane derivatives to establish the factors responsible for the regiochemistry of addition to unsymmetrical cyclopropanes and the reaction trajectory for the addition of both electrophile and nucleophile. It is generally believed that the direction of bond cleavage in such reactions can be accounted for by a modified version of Markovnikov's rule' which states that the ring opens between the carbons bearing the largest nlimber and smallest number of alkyl substituents. However for almost all systems that have been studied a substantial proportion of product results from rupture of the most substituted carbon-carbon bond of the cyclopropanea2 In some instances there are no products resulting from cleavage to the least substituted carbon of a substituted cy~lopropane.~To date no satisfactory explanation has been advanced for the varied behavior observed in cyclopropane ring opening. In all cases of addition to and rearrangement of cyclopropanes the nucleophile, whether external such as solvent or an internal adjacent u bond in the molecular framework, always becomes attached or involved with the most substituted carbon of the cyclopropyl ring. Wiberg" has noted that while relief of steric strain for acid-catalyzed addition to cyclopropane does not correlate with reaction rate, the reaction develops toward the more stable carb~cation.~ The products are considered to be formed by capture of the protonated cyclopropane before it has become an open carbocation, thereby accounting for stereoselective capture by nucleophile, stereoselective migration, or proton loss. The preference for inversion of configuration at the site of nucleophilic attack in addition to cyclopropanes is consistent with the activation barrier from the reaction intermediate to a classical cation being greater than the barrier to nucleophilic attack at the intermediate with inversion. When the cyclopropane is in a rigid skeleton, the ability of a Q bond to overlap with retention (syn-periplanar) or inversion (anti-periplanar) with the cyclopropyl bond undergoing cleavage plays a significant role in determining reaction course.2 The present study reports the electrophilic opening of 2-exo-methyl-endo-tricyclo[3.2.1.0z~4]octane (1) and 2-exo-methyl-endo-tricyclo[3.2.1.02"]oct-6-ene

(12). A previous study of exo- and endo-tricyclo[ 3.2.1.0214]octane3s6and tricycle[ 3.2.1.O2v4]oct-6-ene' has

pointed to the importance of the carbon skeleton on the course of the reaction. The endo-tricyclo[3.2.1.02~4]~ctane in contrast to the exo isomer reacts with acid and mercuric acetate exclusively by rupture of the internal cyclopropyl bond. Intramolecular capture of the developing C4 cation with retention dominates the course of the acid-catalyzed reaction and the trajectory of the proton is toward the corner at C2 which results in inversion of configuration at this center in the reaction. Mercuric acetate addition occurs without skeletal rearrangement competing with external nucleophilic addition of solvent. Since the products of cyclopropane opening are considered to be formed by capture of the protonated cyclopropane before it has become an open carbocation the presence of the methyl in the hydrocarbon 1 and 12 should move the transition-state structure to a more classical carbocation. Such a shift would be expected to affect the stereospecificity of nucleophilic attack. We were therefore interested to establish if the reactions of 1 and 12 with electrophilic reagents proceed by way of a tertiary carbocation with the possibility for interaction with the *-system in hydrocarbon 12 or if residual bridging to C4 dictates the course of reaction. Results and Discussion Protonation and Mercuration of 2-Methyl-endotricyclo[3.2.1.02~4]octane (1). Reaction of 1 with methanol in the presence of catalytic quantities of p-toluenesulfonic acid at room temperature for 4 days gave 2-exo-methoxy-2-endo-methylbicyclo[ 3.2.11octane8p9 (5a, 32 ?& ), 2endo-methoxy-2-exo-methylbicyclo[3.2.1]octane'0 (3a, 31%) (1:l exo/endo attack) and 2-methylbicyclo[3.2.1]oct-2-ene" (6a, 18%). The ethers 5a and 3a are stable (6) Coxon, J. M.; Steel, P. J.; Whittington, B. I.; Battiste, M. A. J.Org. Chem. 1989, 54, 1383. (7) Coxon, J. M.; Steel, P. J.; Whittington, B. I. J. Org. Chem. 1989, 54, 3702. (8) The NMR spectrum was assigned by comparison with the and a heteronuclear known 2-endo-methylbicyclo[3.2.1]octan-2-exo-o19 correlation experiment allowed assignment of the chemical shifts of the protons. (9) Lippmaa, E.; Pehk, T.; Belikova, N. A.; Bobyleva, A. A.; Kalinichenko, A. N.; Ordubadi, M. D.; Plate, A. F. Org. Magn. Reson. 1976,8, 74.

(1) Zimmerman, M. P.; Li, H.-T.;Duax, W. L.; Weeks,C. M.; Djerassi, 1984,106, 5602. C. J . Am. Chem. SOC. (2) Battiste, M. A.; Coxon, J. M. In The Chemistry of the Cyclopropyl Group; Rappoport, Z., Ed.; Wiley and Sons: New York, 1987; Chapter 6, p 255. (3) Coxon, J. M.; Steel, P. J.; Whittington, B. I.; Battiste, M. A. J . Am. Chem. SOC.1988, 110, 2988. ( 4 ) Wiberg, K. B.; Kass, S. R.; de Meijere, A.; Bishop, K. C. J . Am. Chem. SOC.1986. 107. 1003. (5)At the product forming activated complex the structure is considered not to have relaxed to a large extent.2

(10) The 13CNMR spectrum of 3a was assigned by comparison with The the reported spectrum of 2-exo-methylbicyclo[3.2.l]octan-2-endo-ol? previously reported shifts for C3 and C4 in this alcohol are reversed, as shown by the presence of a triplet at 29.6 ppm for the C4 and apparent absence of a peak at 33.7 ppm due to the DS-ero,DS-endo in 2-exomethyl-3,3,4-exo-trideuteriobicyclo[3.2.1]octan-2-endo-ol, 7a. The carbon-hydrogen connectivities of 3a were determined from a heteronuclear correlation experiment. A difference NOE spectrum established the exo stereochemistry of the C2-methyl: irradiation of the methyl a t 1.20 ppm 3.2%), 1.28 (HEs, 3.3%), and gave enhancements at 3.17 (OMe), 2.15 (Hl, 1.45 ppm (H4-ex0, 2.6%).

J. Org. Chem., Vol. 55, No. 13, 1990 4137

Electrophilic Attack on Trisubstituted Cyclopropanes

Scheme 111. Rearrangement of Products from the Reaction in Methanol-d, at of 2-Methyl-endo-tricyclo[3.2.1.02~4]octane

Scheme I. Reaction of 2-Methyl-endo-tricyclo[3.2. l.0a*4]octanewith H+(D+)and Hg(OAc)2at 25 "C

2

1

3

1-

E Hg(0Ac) 18%'

E = D 97%'

80 "C

E-D 3P/o E = HgOAc 9G%

1 -

E-D 41% E HNAc 1 W o

(a) E = H (b) E = D

2

(cj E = HgOAc (d) E = HgSCN

E 11

*estimatedsee text

E- D

P/.

E - HgOAc

0%

Scheme 11. Preparation of the Epimeric 3,3,4-exo-Trideuterio-2-methoxy-2-methylbicyclo[ 3.2.lloctanes

Table I. Stability of the Primary Reaction Products to Methanol and p-Toluenesulfonic Acid at 80 O C

A hD a;+

reactant 3:5 (9:l) 3:5 (32:68)

(i) (ii) MeMgl, NaNHz,EtzO Me1

I

.. H

I

H

D a) R - H b) R - M e

7

y

D

8

under the reaction conditions indicating the ratio is kinetic in origin, and that 6a does not, at room temperature, arise from the ethers. To determine the reaction pathway for the methanol addition to 1 the chemical shifts of the C4 protons for each of the primary reaction products 3a, 5a, 6a had to be unambiguously assigned. To achieve this, authentic deuterio isomers 7b and 8b of the epimeric 2-methoxy-2methylbicyclo[3.2.1]octanes were synthesised (Scheme II).l2 Authentic samples of 3a and 5a were similarly (11)The identity of 6a followed by comparison with the reported lSC NMR spectrume and by preparation of an authentic sample. (12) A heteronuclear correlation spectrum of the epimeric ethers 7b and 8b showed for 7b a triplet in the carbon dimension at 29.4 ppm exhibiting connectivity with a proton at 1.42 ppm. The presence of a triplet in the carbon dimension arises from the C4-exo-D coupling, C4 exhibiting connectivity with only H4-endo at 1.42 ppm due to the high deuterium incorporation at C4-exo. Thus the chemical shift of H4-endo in 3a is established as 1.42 coincident with H4-exo. In addition a 2H NMR spectrum of 4 - e . ~and 4-endo-deuterio-2-endo-methoxy-2-exomethylbicyclo[3.2.1]octane,prepared from the nonspecific NaBD, reduction of 4-endo-(acetoxymercurio)-2-endo-methoxy-2-exo-methylbicyclo[3.2.l]octane,showed a single peak at 1.41 ppm due to D4-exo and D4-endo. For ab,the heteronuclear correlation spectrum showed a triplet in the carbon dimension at 28.3 ppm, exhibiting connectivity with H4endo at 1.26 ppm. As with 7b, the triplet in the carbon dimension arises from the C4-exo-D coupling, no connectivity being observed between C4 and H4-exo due to the high deuterium incorporation at this position.

4

reaction time 26 ha 8 days" 25 h" 8 days" 8 daysb

6 92 67 23 69 28

product ratios 11 3 4 16 8 7 43 16 8 2 36

5 2 9 36 8 34

"[H+] = 0.115 M. b [ H + ] = 0.01 M.

prepared from bicyclo(3.2.l]octan-2-one. For 5a, the chemical shifts of the H4-endo and H4-exo are established as 1.26 and 1.65 ppm, respectively. For 6a,the chemical shifts of H4-exo and H6endo are determined as 2.30 and 1.75 ppm, re~pective1y.l~ To observe the effect of temperature on the reaction course and the preference for thermodynamic control vs kinetic control, 1 was reacted with methanol p-toluenesulfonic acid at 80 OC for 7 days. In addition to the previously observed 6a (53%), 3a (18%),and 5a (21%), 2methoxy-l-methylbicyclo[2.2.2]octane14(1la) (8%) was also present (Scheme 111)and was isolated by preparative GLC. The stability of the primary reaction products (from (13) The mixture of epimeric alcohols 7a and 8a was dehydrated by heating with KHSOl at 160 OC for 30 min (Petit, F.; Evrard, M.; Blanchard, M. Bull. SOC.Chim. Fr. 1971, 4176) to yield %methylbicyclo[3.2.l]oct-2-ene,with deuterium present at C3 (5.05 ppm, 25%), C4-exo (2.30 ppm, 53%), C4-endo (1.75 ppm, 29%) and the methyl (1.65 ppm, 0.40 excess deuterium). A heteronuclear correlation spectrum of this compound shows in the carbon dimension, a triplet at 36.5 ppm exhibiting connectivity with H4-endo at 1.75 ppm, no connectivity with H4-exo being observed due to the higher deuterium incorporation at this position. (14) The partial 'H NMR spectrum of Z-methoxy-l-methylbicyclo[2.2.2]octane has been reported (Kraus, W.; Chassin, C. Tetrahedron Lett. 1970,1113)and is consistent with that observed here. The 'SC NMR spectrum was assigned from the predicted effect of a methoxy group on the lSC NMR spectrum of l-methylbicyclo[2.2.2]octane;Pehk, T. I.; Lippmaa, E. T.; Sokolova, I. M.; Vorob'eva, N. S.; Gervits, E. S.; Bobyleva, A. A.; Kalinichenko, A. N.; Belikova, N. A. Zh.Org. Khim. 1976,12,1201.

4138 J. Org. Chem., Vol. 55, No. 13, 1990 Table 11. Excess Deuterium from the Acid-Catalyzed Addition of Methanol-dl to 2-Meth~l-endo-tricsclor3.2.1.0~~~loctane at 80 "C comDd 6

3 5

D4-endo 98

Coxon et al. Scheme IV. Reaction of 2-Methyl-endo-tricyclo[3.2.1.0z+4]oct-6-ene with H+(D+)and Hg(OAc)z

excess deuterium (atom 70) D3-exo D3-endo methyl 82 ___ 246 243 220 221 251 12

the reaction at room temperature) under the more vigorous conditions was tested by separately reacting each of the compounds in methanol p-toluenesulfonic acid a t 80 "C (Table I). The products interconvert with time a t this higher temperature with the gradual appearance of 1 la; this behavior is consistent with 6a, 3a, and 5a being primary products of reaction. To determine the stereochemistry of proton attack, the reaction of 1 with methanol-dl p-toluenesulfonic acid was examined at 25 "C, and the products were separated by preparative GLC and investigated by NMR. For deuterated 6b, the presence of a triplet in the 13CNMR spectrum at 36.3 ppm and a peak in the 2H NMR spectrum at 1.75 ppm indicated the deuterium stereochemistry a t C4 as endo. For 5b, the presence of a triplet in the 13C NMR spectrum at 28.6 ppm and a peak in the 2H NMR spectrum at 1.23 ppm similarly defined the deuterium stereochemistry at C4 in this compound as endo. However, while the 13C NMR spectrum of 3b indicated the presence of the C4 deuterium by the presence of a triplet at 29.7 ppm, the unfortunate coincidence12 of the chemical shifts of the 4-ex0 and 4-endo protons (and hence deuterons), means the deuterium stereochemistry at C4 is indeterminate. To ascertain the stereochemistry of C4-D in 3b, a 76:24 mixture of 3b and 5b, obtained by preparative GLC from the reaction of 1 with methanol-d, at room temperature, was reacted with methanol p-toluenesulfonic acid at 80 "C for and 13C NMR analyses 32 h. GLC and subsequent 'H,2H, confirmed the presence of 4-endo-deuterio-2-methylbicyclo[3.2.l]oct-2-ene (6b) (57%) in a mixture with 5b (19%) and 3b (23%). The presence of triplets in the 13C NMR spectrum of the crude reaction mixture corresponding to C4-D for each of 3b, 5b, and 6b and the presence of peaks in the 2H NMR spectrum at 1.72 (6b), 1.40 (3b), and 1.23 ppm (5b) along with the absence of peaks corresponding to 4-exo-deuterio-2-methylbicyclo[ 3.2.lIoct-2-ene (2.27 ppm) and 4-exo-deuterio-2-exomethoxy-2-endo-methylbicyclo[3.2.1]octane(1.62 ppm) indicates the deuterium stereochemistry a t C4 in 3b as endo.15 The observation of C4-endo-D in all three of the primary reaction products from the reaction of 1 with methanol-d, at room temperature is consistent with corner attack by proton (deuteron) at the cyclopropyl ring. This reflects either an inherent preference for protonation a t C4 as compared to C3 or that subsequent reaction at the C4-protonated cation is more facile than reaction at the C3-protonated cation. The reaction of 1 with methanol-d, p-toluenesulfonic acid a t 80 "C for 7 days yielded deuterated 2-methylbicyclo[ 3.2.11oct-2-ene (6), 2-exo-methoxy-2-endomethylbicyclo[3.2.1]octane (5), 2-endo-methoxy-2-exomethylbicyclo[3.2.1]octane (3),and 2-methoxy-1-methylbicyclo[2.2.2]octane (11)in a similar ratio to that previously obtained. The deuterium distribution obtained from mass spectral analysis and 2H and 13CNMR spectra (Table (15) Resolution of the 4-ex0 and 4-endo deuterons in the product from nonspecific NaBD, reduction of 4-endo-(acetoxymercuio)-2-endo-methoxy-2-ero-methylbicyclo[3.2.l]octaneby the use of Eu(fod)3shift reagent was unsuccessful.

13

I

E = D 85%'

E-D14%'

f

/

t

15

-

E D 27%'

I

14 E-D 29% E-HgOk82%

-

16

E- D E

44% HgOk 11%

(a)E=H (b) E = D (c) E = HgOAc estimated see text

17

18 E-D 27% E HgoAc 7%

-

11) is consistent with the multiple addition/elimination mechanism shown in Scheme 111. The observation of a deuterium a t C5-anti and not C5-syn of deuterio 11 requires nucleophilic attack at the bridged cation 10 to occur before relaxation to the free carbocation. The deuterium incorporation at C3 and the methyl in each of the compounds arises from repeated methanol addition to 6 and 10 and elimination from the epimeric ethers 3 and 5.16 In contrast to the acid-catalyzed addition of methanol, reaction of 1 with mercuric acetate in methanol yields, after sodium mercury amalgam reduction in sodium hydroxide, a 9:l mixture of 3a and 5a, respectively."J8 Stereospecific r e d u ~ t i o n of ' ~ the organomercurial mixture with sodium amalgam in sodium deuteroxide gave a 93:7 mixture of the 4-endo-deuterio-2-methoxy-2-methylbicyclo[3.2.l]octanes 3b and 5b. The observation of C4-endo deuterium in 5b from stereospecific reduction of 5c with sodium amalgam in NaOD and a 4-exo-H in 3c defined the stereochemistry (16) The W e n d o deuterium arises from initial deuteron attack with inversion at the cyclopropyl ring. (17) Separation was achieved by preparative GLC, and the products were identical to those from the acid-catalyzed methanol addition at room temperature. (18) While the intermediate organomercurial mixture was not separated, the major component of this reaction, 3c, was present in sufficient guantity (ca.90%) to allow the determination of apectroscopic data The C-'%Hg couplings support a 4-endo-acetoxymercuriogroup. The axial nature of the C4H and hence the configuration of the acetoxymercurio group in 3c was further confirmed by proton-proton couplings (selective decoupling) to the C3-endo-H (13.6 Hz),C3-em-H (5.2 Hz), CG-ero-H (1.5 Hz), and C5H (1.5 Hz). A difference NOE spectrum, performed on the mixture (91) of the thiocyanatomercurials 3d and 5d,showed that irradiation of the methyl group at1.20 ppm gave enhancements at 3.18 (OMe, 5.1%), 2.91 (H4-ex0, 5.6%), 2.07 (Hl, 2.8%), 1.96 (H3-exo, 3.2%), and 1.56 ppm ( H ~ s3.5%), , thereby confirming the exo stereochemistry of the methyl and hence the endo nature of the methoxy group. (19) Kitching, W.; Atkins, A. R.; Wickham, G.;Alberts, V. J . Org. Chem. 1981, 46, 563.

Electrophilic Attack on Trisubstituted Cyclopropanes

of the mercuric acetate attack on 1 as at the corner with inversion, the reaction occurring without skeletal rearrangement. Protonation and Mercuration of 2-Methyl-endotncyclo[3.Z.1.0z~4]oct-6-ene (12). The acid-catalyzed reaction of 12 with methanol at roan temperature for 3 days (87% reaction) gave three comnounds. 14a?O 16a."' and in the raGo 293833, respectivelyz3 (Scheme IV). While 14a was stable under the reaction conditions, 16a gave 18a along with 16a in the ratio of 1:9. The greater reactivity of 16a relative to 14a reflecta the relationship of the double bond to the exo-methoxygroup. Ether l!ja gave a 1:l mixture of 16a and Ma after 22 h, a product ratio subsequently invariant for 21 days." The solvolysis of 18a is consistent with the intermediacv of cation 17a. nucleophilic attack on this species givingl6a and 18a in the ratio 1:l. Stereoselective exo attack in the solvolysis of 18a indicates nucleophilic attack on the classical tertiary cation 15, if it is indeed present in the solvolysis reaction, is not competitive with attack on 17. The reaction of 12 with mercuric acetate in methanol, and subsequent sodium amalgam reduction with sodium hydroxide, gave 14a (SZ%), 168 (ll%), and 18a (7%) identical with those previously obtained from the acidcatalyzed methanol addition at 25 'C. Hydrogenation of the crude reaction mixture gave a mixture containing mainly 3a identical with an authentic sample. While the original organomercurial mixture was not able to be separated, 14c was present in sufficient yield to allow determination of its spectroscopic dataF5 To confirm the

J. Org. Chem., Vol. 55, No. 13, 1990 4139

Me

H

v

- -

e, Figure 1. Mixing of C1,CB and C5,CBorbitals with cyclopropane orbitals showing interaction with electrophilesat comer and edge. er

stereochemistry of the acetoxymercurio group, a sodium amaleam reduction of the crude oreanomercurial mixture in so&um deuteroxide was carriei out to give 14b, 16b, and 18b. The major component 14b was separated by preparative GLC and the presence of a Cbendedeuterium after the stereospecific reduction was confirmedz6by the presence of a triplet in the NMR spectrum at 22.6 ppm and the loss of a coupling from H4-endo to H8a (1.7 Hz) and H3-endo (3.6 Hz). The deuterium stereochemistry in 16b was similarly established as Ckendo due to the NMR spectrum at 21.7 ppm presence of a triplet in the and a peak in the ZHNMR spectrum at 1.20 ppm corresponding to CCendo-deuterium. While the deuterium stereochemistry in 18b was not determined it would be expected, by comparison with 14b and 13b that the deuterium be C4-endo. Given the stereaspecific nature of the organomercurial reduction, it is therefore apparent that the mercuric salt attacks the cyclopropane ring with inversion of configuration to give 14c and 16c, and by implication, 18c. The higher degree of unrearranged product (20)The identity of l4a was established by methods similar to those described for 168. 14c as compared to the reaction with proton (deuteron) (21) The identity of 16. was established from spectral studies and by is indicative of the lack of substantial charge development hydrogenation to 51. The 'H NMR SPeCtNm of 16a me assigned by - ~ 1reaction with mercuric acetate. comparison with that of 2 - e n d o - m e t h y l h i e y c l o [ 3 . 2 . 1 1 ~ ~ 6 ~ ~ ~ - 2 - ~in~ ~the Bohlmann, F.; Rotard, W.Justus Liebigs Ann. Chem. 1982,1220 and by To determine the stereochemistry of proton attack on selective decoupling and difference NOES. In particular, the e m sterethe cyclopropane ring, the acid-catalyzed addition of ochemistry of the methoxy methyl follows from a difference NOE speemethanol-d, to 12 was examined at room temperature. trum. Irradiation of H8s (1.95 ppm), so assigned due to a coupling with H8a (1.72 ppm, 10.0 Hz) and lack of coupling with H1/H5, gives enReaction for 7 days (79% reaction) gave 14b,2?16b, and hancements a t the methoxy methyl (3.19 ppm, 0.8%), H l l H 5 (2.54 ppm, 18b in the ratio 294427, respectively. For product 16b, 1.0%). H8s (1.72 ppm, 12.5%), H4.exo (1.62 ppm, 2.5%), and the methyl the presence of a triplet in the 'T NMR spectrum at 21.7 (1.03 ppm, 0.4%). A heteronuclear correlation experiment identified connectivities between, m o n g 0th" H4-ex0 1.62 ppm and H4-end0 1.23 ppm and a peak at 1.22 ppm in the ZHNMR spectrum ppm/C4,22.2 ppm and H8s 1.95 ppm and H8a 1.72 ppmlC8.38.8 ppm. along with the loss of a coupling from H8a (1.72 ppm) to A coupling between C4H a t 1.23 ppm and H8a of 2.3 Hz confirms the H4-endo (2.3 Hz)is consistent with a C4-endo-D. For 18b assignment of this proton as C4-endo-H. (22) The identity of 188 was determined as follows. Comparison with the presence of a Ckendo deuterium similarly follows from the 'H NMR SpeCtNm of 6-exo-methoxytri~yelo[3.2.l.ff~~Imtm~~ me& the presence of a triplet in the NMR spectrum at 25.4 a Iws of coupling of ea. 7 Hz from the cyclopropyl proton a t 1.3 ppm, ppm and a peak in the 2H NMR spectrum at 1.32 ppm in indicating the methyl is substituted at the cycloprapyl ring. A difference addition to a loss of a 2.1-Hz coupling from HSa (1.82 ppm) NOE spectrum further established the methyl to be a t C2. Irradiation of the methyl at 0.92 ppm gave enhancements a t H3-exoIH3-endo to H4-endo. (1.66-1.60 ppm. 2.2% total), H7 (1.30 ppm. 6.4%), and H I (1.19 ppm, The HOMO and subjacent orbital of 1 will contain a 5.0%). The methoxy group was established to he a t C6-exo hy eomparcontribution from the Cl,CS/CS,CS u bondsz8with the ison with the couplings a t the C6-H observed for 2-methyltricyclo[3.2.1.0z~'loctan-6-exo-ol.z'H6-endo for both these compounds appears cyclopropane e. and e. orbitals. An unfavorable secondary in the 'H NMR spectrum as B singlet, while for 2-methyltricyclo[3.2.1.0"'loctan-6endo-ol, H6-ex0 appears as a quartet with couplings of 4.5 and 4 0 Hz to H5 and HT. respe&rly. A difference NOE